Huang Juan, Guo Xiaofeng, Ji Wei
Department of Cardiology, Fujian Provincial Children's Hospital, Fuzhou, Fujian 350011, China.
Zhonghua Yi Xue Yi Chuan Xue Za Zhi. 2023 Sep 10;40(9):1165-1170. doi: 10.3760/cma.j.cn511374-20220928-00652.
To explore the clinical and genetic characteristics of a child with Arrhythmogenic right ventricular cardiomyopathy (ARVC).
A 6-year-old boy with ARVC who had visited Fujian Provincial Children's Hospital on August 23, 2022 was selected as the study subject. Relevant clinical data were collected, and peripheral venous blood samples were collected from the child and his parents for genetic testing through whole exome sequencing (WES). Sanger sequencing was carried out for family verification, and pathogenicity analysis was conducted for the candidate variants.
The child had exhibited clinical symptoms including systemic edema, generalized heart enlargement, universal reduction of interventricular septum and ventricular wall movement, reduced left ventricular diastolic and systolic function, and reduced right ventricular systolic function. WES revealed that the child has harbored compound heterozygous variants of the PKP2 gene, namely c.119_122del (p.Leu40ArgfsTer71) and c.1978G>A (p.Gly660Arg), which were verified by Sanger sequencing to be respectively inherited from his father and mother. The c.119_122del variant has not been recorded in the 1000 Genomes, gnomAD and ExAC databases, and was predicted to lead to truncation of the PKP2 protein by SWISS-MODEL and PyMOL online software and classified as likely pathogenic based on the guidelines jointly developed by the American College of Medical Genetics and Genomics (ACMG) and ClinGen. The c.1978G>A variant has also not been recorded in the 1000 Genomes, gnomAD and ExAC databases, and was predicted to be deleterious by online software including REVEL, SIFT, CADD, Mutation Taster, and PolyPhen-2. The amino acid encoded by the variant site was highly conserved among various species by analysis using T-coffee and ESPript v3.0 online servers. The variant may affect the protein function by SWISS-MODEL and PyMOL online server analysis, and was classified as likely pathogenic based on the guidelines jointly developed by the ACMG and ClinGen.
The compound heterozygous variants of c.119_122del (p.Leu40ArgfsTer71) and c.1978G>A (p.Gly660Arg) of the PKP2 gene probably underlay the ARVC in this child. Above finding has broadened the spectrum of PKP2 gene variants and provided a reference for the diagnosis and genetic counseling.
探讨一名致心律失常性右室心肌病(ARVC)患儿的临床及遗传特征。
选取一名于2022年8月23日就诊于福建省儿童医院的6岁ARVC男孩作为研究对象。收集相关临床资料,并采集患儿及其父母的外周静脉血样本,通过全外显子组测序(WES)进行基因检测。采用Sanger测序进行家系验证,并对候选变异进行致病性分析。
该患儿出现的临床症状包括全身性水肿、全心扩大、室间隔及心室壁运动普遍减弱、左心室舒张和收缩功能降低以及右心室收缩功能降低。WES显示该患儿携带PKP2基因的复合杂合变异,即c.119_122del(p.Leu40ArgfsTer71)和c.1978G>A(p.Gly660Arg),经Sanger测序验证分别遗传自其父亲和母亲。c.119_122del变异未在千人基因组、gnomAD和ExAC数据库中记录,经SWISS-MODEL和PyMOL在线软件预测会导致PKP2蛋白截短,并根据美国医学遗传学与基因组学学会(ACMG)和临床基因组资源(ClinGen)联合制定的指南分类为可能致病。c.1978G>A变异也未在千人基因组、gnomAD和ExAC数据库中记录,经包括REVEL、SIFT、CADD、Mutation Taster和PolyPhen-2在内的在线软件预测具有有害性。通过使用T-coffee和ESPript v3.0在线服务器分析,变异位点编码的氨基酸在不同物种间高度保守。经SWISS-MODEL和PyMOL在线服务器分析该变异可能影响蛋白质功能,并根据ACMG和ClinGen联合制定的指南分类为可能致病。
PKP2基因的c.119_122del(p.Leu40ArgfsTer71)和c.1978G>A(p.Gly66Int)复合杂合变异可能是该患儿ARVC的病因。上述发现拓宽了PKP2基因变异谱,为诊断和遗传咨询提供了参考。
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